Mesothelioma Clinical Trial Evaluating Selecta’s SEL-403 Begins

Selecta Biosciences, a clinical-stage biopharmaceutical company, and the National Cancer Institute (NCI) teamed up for the phase 1 clinical trial under the Cooperative Research and Development Agreement.

The trial will evaluate safety and tolerability of SEL-403, Selecta’s investigational new drug combination consisting of a potent anti-tumor agent (LMB-100) and a drug that prevents an immune response (SVP-Rapamycin).

LMB-100 and SVP-Rapamycin have been studied separately in clinical trials. Researchers hope combining the two therapies will improve effectiveness and increase the number of treatments patients can receive before there is an antibody response and the LMB-100 portion stops working.

The U.S. Food and Drug Administration accepted an investigational new drug application for SEL-403 in January.

“Mesothelioma remains one of the deadliest and most challenging-to-treat forms of cancer,” Dr. Raffit Hassan, principal investigator of the trial and senior investigator at NCI’s Center for Cancer Research, said in a press release. “We are pleased to get this clinical investigation underway to determine if patients may indeed benefit from a combination therapy consisting of LMB-100 and SVP-Rapamycin.”

“We feel very blessed to have the opportunity at this trial and wish the best for everyone who is undergoing some kind of experimental treatment,” Pam said. “Let’s hope [Selecta] is successful so they keep this drug on trial and hopefully as a new, hopeful treatment.”

Jim received his first cycle of SEL-403 in early March and is back at NCI this week for the second cycle. Each treatment cycle consists of an initial dose of the LMB-100 and SVP-Rapamycin combination on the first day, followed by LMB-100 alone on the third and fifth day.

“We won’t know until the CT scan at the end of April if this is working,” Pam said. “But so far the study doctors are pleased with how the drug is circulating and seems to be getting to the tumor sites.”

A known side effect of LMB-100 is systemic capillary leak syndrome (SCLS), a condition in which fluid and proteins leak out of tiny blood vessels into surrounding tissues. Jim has shown signs of SCLS since he began treatment, requiring a trip to the emergency room.

“It made him very short of breath, oxygen levels dropped and fluid built up around his body,” Pam said. “But our home oncologist is working close with the [NCI] team to keep him on medicine to flush the fluid out and he is now improving.”

Pam urges others undergoing experimental treatments to alert their local oncologist of the trial and have an emergency contact list and protocol document from the study ready in case an ER visit in necessary.

“That saves you from wasting precious time with an ER staff who knows nothing of the cancer or protocol,” she said.

SEL-403 Attacks Cancer While Suppressing Immune System

The trial, held at NCI in Bethesda, Maryland, is expected to enroll up to 18 patients.

The study will evaluate the safety and tolerability of the drug in addition to providing data on pharmacokinetics, anti-drug antibody (ADA) levels and overall response rate.

LMB-100 is an immunotoxin that targets mesothelin, a protein overexpressed in 90 percent of mesothelioma cases.

Immunotoxins can be designed to block the synthesis of proteins inside cancer cells, causing the cells to die while minimizing off-target side effects.

Unfortunately, because immunotoxins are foreign proteins, they produce a high immune response. This lowers the efficacy of the drugs and until now has restricted their use as a cancer treatment.

By adding SVP-Rapamycin, SEL-403 is designed to avoid this immune response, which could enable prolonged immunotoxin dosing and enhanced anti-tumor activity.

“Immunotoxins have long been viewed as a drug class that could profoundly impact the treatment paradigm of both solid tumors and blood-borne cancers,” Werner Cautreels, president and CEO of Selecta, said in a press release. “With our SEL-403 product candidate, which combines our proprietary SVP-Rapamycin technology with LMB-100, we believe the potential exists to avoid immunogenicity, thereby allowing patients to receive multiple treatment cycles and benefit fully from treatment.”

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Matt Mauney is an award-winning journalist with nearly a decade of professional writing experience. He joined Asbestos.com in 2016, and he spends much of his time reading, analyzing and reporting on mesothelioma research articles to ensure people in the mesothelioma community know the latest medical advancements. Prior to joining Asbestos.com, Matt was a reporter at the Orlando Sentinel. Matt also edits some of the pages on the website. He also holds a certificate in health writing from the Centers for Disease Control and Prevention. Read More

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